| Literature DB >> 33860195 |
Bjoern Papke1, Salma H Azam1,2, Anne Y Feng1, Christina Gutierrez-Ford1, Hayden Huggins1,2, Pradeep S Pallan3, Amanda E D Van Swearingen1, Martin Egli3, Adrienne D Cox1,4,4, Channing J Der1,4, Chad V Pecot1,1,4,4.
Abstract
Oncogenic mutations in the KRAS gene are well-established drivers of cancer. While the recently developed KRASG12C inhibitors offer a targeted KRAS therapy and have shown success in the clinic, KRASG12C represents only 11% of all KRAS mutations. Current therapeutic approaches for all other KRAS mutations are both indirect and nonmutant-selective, largely focusing on inhibition of downstream KRAS effectors such as MAP kinases. Inhibition of KRAS downstream signaling results in a system-wide down-modulation of the respective targets, raising concerns about systemic cell toxicity. Here, we describe a custom short interfering RNA oligonucleotide (EFTX-D1) designed to preferentially bind mRNA of the most commonly occurring KRAS missense mutations in codons 12 and 13. We determined that EFTX-D1 preferentially reduced the mutant KRAS sequence versus wild-type at the levels of both transcription and translation and reversed oncogenic KRAS-induced morphologic and growth transformation. Furthermore, EFTX-D1 significantly impaired the proliferation of several KRAS mutant cancer cell lines in 2-D as well as 3-D assays. Taken together, our data indicate a novel use of RNA interference to target oncogenic KRAS-driven cancers specifically.Entities:
Year: 2021 PMID: 33860195 PMCID: PMC8033609 DOI: 10.1021/acsptsci.0c00165
Source DB: PubMed Journal: ACS Pharmacol Transl Sci ISSN: 2575-9108